What question did this study set out to answer?

The aim is to understand how IL-33 protects against sepsis-induced liver injury.

January 25, 2026

IL-33 Alleviates Sepsis-Induced Liver Injury by Regulating theNF-κB/BCL-2 Pathway

Key Points

The aim is to understand how IL-33 protects against sepsis-induced liver injury.
Modeled sepsis-induced liver injury using cecal ligation and puncture in vivo and LPS stimulation in vitro
Performed oxidative stress analysis and inflammatory cytokine measurements
Examined liver function biomarkers and histomorphological studies
Investigated IL-33 signaling through transcriptomic analysis and pharmacological interventions
Exogenous IL-33 preserved liver architecture and function while reducing inflammation and oxidative damage.
Blocking IL-33 signaling with anti-ST2 intensified hepatocellular damage.
IL-33/ST2 stimulation suppressed NF-κB pathway activity, increased BCL-2 expression, and inhibited apoptosis.

Abstract

Background: Interleukin-33 (IL-33), a tissue-derived alarmin released during sterile and infectious stress, modulates inflammatory responses in an organ-specific manner. Although IL-33 is implicated in hepatic pathophysiology, its functional mechanism in sepsis-induced liver injury (SILI) remains insufficiently characterized. Method: SILI was modeled in vivo via cecal ligation and puncture (CLP) and in vitro using lipopolysaccharide (LPS)-stimulated primary hepatocytes. The multimodal evaluations included oxidative stress analysis, inflammatory cytokine measurements, liver functional biomarker analysis, and histomorphological studies. IL-33 signaling was investigated by combining transcriptomic pathway analysis with pharmacological interventions with soluble ST2 decoy receptor (sST2) and ST2-neutralizing (anti-ST2) antibodies. The SILI model dynamically increased the IL-33 level. Results: Exogenous IL-33 conserved liver architecture, improved function, and reduced both inflammation and oxidative damage. Critically, blocking IL-33/ST2 signaling with an anti-ST2 antibody or sST2 eliminated the protective effect of IL-33, worsening hepatocellular damage. Mechanistic investigations revealed that IL-33/ST2 stimulation reduced NF-κB pathway activity, improved BCL-2 expression, and inhibited caspase-3-- mediated apoptosis. The lack of the antiapoptotic effects of IL-33 on NF-κB pathway activation validated its regulatory axis specificity. Discussion: This study identifies IL-33/ST2-NF-κB-BCL-2 as a key axis mitigating hepatocyte apoptosis in SILI. IL-33-based therapies may offer dual control of inflammation and cell death, though clinical translation requires temporal optimization. Conclusion: Our results suggest that the pharmacologically targeted IL-33/ST2-NF-κB-BCL-2 pathway decreases sepsis-induced hepatocyte apoptosis. These findings indicate that IL-33-based treatments may be feasible for treating SILI and that this axis coordinates cytoprotection by concurrently controlling inflammatory signals and apoptotic processes.

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Cite This Study

Wu et al. (Tue,) studied this question.

synapsesocial.com/papers/6975b26ffeba4585c2d6de87 https://doi.org/https://doi.org/10.2174/0109298673423384251128081056

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